Myopalladin knockout mice develop cardiac dilation and show a maladaptive response to mechanical pressure overload.

Myopalladin (MYPN) is a striated muscle-specific immunoglobulin domain-containing protein located in the sarcomeric Z-line and I-band. MYPN gene mutations are causative for dilated (DCM), hypertrophic, and restrictive cardiomyopathy. In a yeast two-hybrid screening, MYPN was found to bind to titin in the Z-line, which was confirmed by microscale thermophoresis. Cardiac analyses of MYPN knockout (MKO) mice showed the development of mild cardiac dilation and systolic dysfunction, associated with decreased myofibrillar isometric tension generation and increased resting tension at longer sarcomere lengths. MKO mice exhibited a normal hypertrophic response to transaortic constriction (TAC), but rapidly developed severe cardiac dilation and systolic dysfunction, associated with fibrosis, increased fetal gene expression, higher intercalated disc fold amplitude, decreased calsequestrin-2 protein levels, and increased desmoplakin and SORBS2 protein levels. Cardiomyocyte analyses showed delayed Ca ²⁺ release and reuptake in unstressed MKO mice as well as reduced Ca ²⁺ spark amplitude post-TAC, suggesting that altered Ca ²⁺ handling may contribute to the development of DCM in MKO mice.
Competing Interests: MF, DY, RM, AG, NP, BS, RC, FD, JZ, AF, SN, SS, CT, DC, WL, RP, CP, MG, MB No competing interests declared, PC The authors declare that no competing interests exist.
(© 2021, Filomena et al.)